Sepsis Clinical Trial
Official title:
Five Percent Albumin Versus Normal Saline as Fluid Resuscitation Strategies for the Management of Early Suspected Septic Shock
Severe infection in the intensive care unit is common accounting for about 10% of admissions
and has a death rate of approximately 40-50%. It is almost always associated with significant
reductions in blood pressure. Administration of fluid often in large volumes is essential to
normalize blood pressure and prevent failure of organs and death. Two common classes of fluid
solutions are crystalloid fluids (salt based, normal saline) and colloid fluids (protein
based, albumin). Due to its properties, the albumin fluid may remain in the vascular space
better than the normal saline solution. Hence, there may be faster attainment of normal blood
pressure as well as a reduction in failed organs and death. Preliminary clinical trial data
suggests a potential for benefit with albumin in this setting but these findings require
confirmation in a large clinical trial.
There are few data to explain how albumin may exert its protective effects and lead to better
outcomes for patients with severe infections. We will conduct a clinical study that will
examine potential biological mechanisms for albumin's protective effects in 50 patients
across 6 Canadian academic hospitals. We will also examine our ability to successfully
recruit patients into this trial.
This study will provide information that will help to understand the biological mechanisms of
albumin in severe infection. The information gained will guide the investigative team for
future fluid related mechanistic questions. The study will also provide essential information
that will aid in the design and conduct of the future large clinical trial that will examine
death as its primary outcome.
Background: Severe sepsis and septic shock are the most common causes of mortality among
critically ill patients and account for approximately 10% of admissions to the intensive care
unit (ICU) and 3% of all admissions to hospital. Despite decades of therapeutic
investigation, mortality of septic shock has remained at approximately 40-50%. Fluid
resuscitation is an integral component of early treatment, as several liters of fluid may be
administered in the first hours of septic shock in an attempt to re-establish hemodynamic
stability. The two main classes of fluid expand the plasma volume include crystalloids and
colloids.
In Canada, the main crystalloid fluids used for resuscitation are normal saline and ringers
lactate; the main colloid fluids used for resuscitation are hydroxyethyl starches (HES) and
albumin. Until recently, no randomized controlled (RCT) or systematic review had confirmed
benefit or harm with either colloidal or crystalloid fluids in this patient population. An
RCT published in 2008 demonstrated that 10% pentastarch (HES fluid) causes acute renal
failure defined by the requirement for renal replacement therapy. In contrast, a subgroup
analysis from a RCT of severe sepsis suggests that 4% albumin fluid may reduce death.
However, these hypothesis-generating findings require confirmation in the context of a large
RCT.
There are limited observational mechanistic studies designed to understand the potential
biological mechanisms for albumin's potential protective effects in sepsis. Moreover,
mechanistic data in the clinical trial setting are lacking. The PRECISE pilot RCT (Five
Percent Albumin versus Normal Saline as Fluid Resuscitation Strategies for the Management of
Early Suspected Septic Shock) will help to understand the biological mechanisms of albumin in
early septic shock and explore feasibility issues in preparation for a large RCT.
Study Hypotheses: We hypothesize that resuscitation with 5% albumin as compared to normal
saline in early septic shock may exert some of its protective effects through the following
biological mechanisms: 1) Limiting thrombin generation, 2) Supporting endogenous protein C
and activated protein C (APC) generation, 3) Limiting the production of systemic
pro-inflammatory cytokines and chemokines and supporting the production of cytokines and
chemokines with anti-inflammatory potential, and 4) Reducing the ability of septic plasma to
generate Neutrophil Extracellular Traps (NETs).
Study Design/Setting: A multi-centre randomized controlled trial conducted in 6 Canadian
academic centres.
Participants: The study will enroll 50 adult patients who are identified with early suspected
septic shock from the emergency department (ED) and the intensive care unit (ICU). Patients
need to be hypotensive or require vasopressor agents, have at least 2 systemic inflammatory
response syndrome criteria, and have no other form of shock (e.g., cardiogenic, obstructive,
or hemorrhagic shock) and no previous ICU admission for severe sepsis or septic shock after
receiving at least 1 litre of crystalloid and not more than 250 mls of colloid fluid within 8
hours of the first hypotensive event.
Interventions: Participants will be randomly assigned to 1 of 2 arms. Patients, families,
clinicians, and research personnel will be blinded to the fluid administered (5% albumin or
0.9% normal saline). Fluid resuscitation will begin immediately after randomization and
continue for the first 7 days or until discharge from the ICU or ED if this occurs sooner.
Blood and urine will be collected at randomization and then at 6, 12, 24, 72 hrs and 7 days
later. Study fluid will be administered as rapidly as possible as 500 ml fluid challenges.
All other co-interventions of care will not be protocolized or mandated during the study
period.
Main Outcome Measures: The primary outcome is a comparison of thrombin generation at 72
hours, and protein C and APC levels at 7 days. Secondary outcomes include a comparison of
inflammatory cytokine and chemokine levels in the blood and urine. Other clinical outcomes
will include mortality in ICU, hospital, and at 30 days, length of stay in ICU and hospital,
development of organ failure, and need for organ support (defined by the number of days
requiring mechanical ventilation and renal replacement therapy) and feasibility measured in
terms of patient recruitment.
Trial Team: The trial will be led by 3 primary investigators (Lauralyn McIntyre, Alison
Fox-Robichaud, and Alan Tinmouth), who will have responsibility for all aspects of the trial.
They have expertise in hematology, transfusion medicine, basic science and clinical trials in
critical care. Our team includes co-investigators from the ICU (Drs. Lauralyn McIntyre, Joe
Pagliarello, Anand Kumar, Sean Bagshaw, Alison Fox-Robichaud, Alexis Turgeon), ED (Drs. Ian
Stiell, Brian Rowe, Andrew Worster, Marcel Emond), and ICU/ED (Drs. Robert Green, David
Easton) who will act as clinical champions at each participating site. Many co-investigators
have extensive experience in the conduct of multi-centre RCTs (Drs. Paul Hebert, Deborah
Cook, Dean Fergusson, John Marshall, Ian Stiell, Brian Rowe, Simon Finfer, Alan Tinmouth,
Lauralyn McIntyre). The translational co-investigative team includes critical care physicians
with expertise in sepsis pathophysiology (Drs. Alison Fox Robichaud, Paul Kubes, Patricia
Liaw, Anand Kumar, John Marshall, Tao Rui, and Claudio Martin).
Significance of findings: Results from our PRECISE pilot RCT may provide a biologic rationale
for a beneficial effect of 5% albumin in early septic shock resuscitation. If a biologic
rationale is confirmed, the study will also provide essential information to determine the
feasibility and aid the design of a definitive phase III trial of albumin in resuscitation of
septic shock.
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